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Abstract

Background

This article provides new insights into the impact of social engagement on CVD risk
factors in older adults. We hypothesized that objective (social participation, social
ties and marital status) and subjective (emotional support) aspects of social engagement
are independently associated with objective measures of cardiovascular risk.

Methods

Data from the English Longitudinal Study on Ageing (ELSA) were analyzed. The effects
of social participation, social ties, marital status, and emotional support on hypertension,
obesity, high sensitivity C-reactive protein, and fibrinogen were estimated by logistic
regression controlling for age, sex, education, physical function, depression, cardiovascular
disease, other chronic diseases, physical activity, and smoking.

Results

Social participation is a consistent predictor of low risk for four risk factors,
even after controlling for a wide range of covariates. Being married is associated
with lower risk for hypertension. Social ties and emotional support are not significantly
associated with any of the cardiovascular risk factors.

Conclusion

Our analysis suggests that participation in social activities has a stronger association
with CV risk factors than marital status, social ties or emotional support. Different
forms of social engagement may therefore have different implications for the biological
risk factors involved.

Background

Cardiovascular disease (CVD) is the leading cause of morbidity and mortality in Europe
(WHO, 2005), accounting for over 4.3 million deaths each year [1], a figure that amounts to nearly half (48%) of all deaths in Europe. Overall CVD
is estimated to cost the EU economy €192 billion a year, of which €110 billion (57%)
is due to health care costs and €82 billion (43%) to productivity losses and informal
care [1].

Evidence from the USA prospective studies has suggested that social engagement lowers
the incidence of cardiovascular disease and other chronic diseases [2-6]. Social engagement has been shown to have a beneficial effect on several behaviours that affect the risk of cardiovascular disease such as smoking [7-9], smoking cessation [10,11], adherence to medical treatment [12], participation in physical activity [13,14] and diet [15,16]. Social engagement also influences health through psychological processes. Social contacts can attenuate stressful experiences by helping to solve
problems, or by giving a new interpretation of adverse events [17], thereby buffering the harmful effects of stress [7,18,19]. Social engagement also modulates cardiovascular reactivity [17] via reduced sympathetic nervous system activity and/or stress-related hormonal activity.
Social engagement which attenuates the neuro-endocrine stress response [7,17], influences one's emotional state, giving a sense of purpose, meaning and belonging
and reducing the intensity and duration of negative affective states [20].

Few studies have examined the possible differential impact of aspects of social engagement
and consequently little is known about which components of social engagement are most
protective for cardiovascular disease [21]. Disciplinary differences in research approaches contributed to this outcome. While
social scientists have focused on "objective" aspects of relationships such as marital
status [22], social networks [2], contact with network members, and participation in social activities [23], psychologists have focused on subjective aspects of social relationships such as
perceived emotional support and loneliness [24]. In addition, data limitations have encouraged researchers to focus on either subjective
or objective aspects of social engagement [25].

In a recent meta-analysis, the protective effects of distinct types of social support
on the incidence and prognosis of coronary heart disease (CHD) were mixed. While there
was evidence that emotional support was protective against the prevalence and disease
progression of CHD, the results were unclear for structural support (defined as number
of contacts, membership of community groups and marital status) [26].

The aim of this paper is to make a contribution to the literature by examining the
effects of social engagement on CV risk factors. Our use of direct measures of health
instead of self-perceived (self-reported) health, is a further improvement from previous
studies, because direct measures reduce the likelihood of reporting bias errors [27].

In this article, 'social engagement' refers to a combination of objective and subjective
measures of the salient aspects of people's 'social' existence. The objective measures
are defined by connectedness to other individuals (the number of children, friends
and relatives whom the respondent feels are close to him/her) and participation in
social groups (affiliation to or membership in religious, voluntary, political, and
social associations or activities). The first, we refer as "social ties", and the
second as "social participation". The subjective measures comprise of perceptions
of available emotional support from spouse, children, relatives and friends. These
components are based on previous studies of older individuals [28]. We hypothesized that objective (social participation, social ties and marital status)
and subjective (emotional support) aspects of social engagement are independently
associated with objective measures of CV risk.

The risk factors examined here have well-established associations with cardiovascular
diseases: hypertension, obesity and two inflammatory markers - fibrinogen, and high
sensitivity C-reactive protein (hsCRP). Epidemiological studies have shown that both
systolic (SBP) and diastolic blood pressure (DBP) are important cardiovascular risk
factors [29]. Obesity, measured by BMI, is an independent predictor of coronary heart disease
[29,30]. Both high sensitivity CRP and fibrinogen are acute phase inflammation reactants.
Prospective studies and meta-analysis have demonstrated that hsCRP [31-34] and fibrinogen [35,36] are strong independent predictors of the risk of cardiovascular disease in healthy
individuals and in those with pre-existing CVD. Specifically, hsCRP is a predictor
of frailty [37], a risk factor for the development of arterial fibrillation [38], ischemic stroke [39], and diabetes [40]. Fibrinogen is involved in thrombogenesis and in the stimulation of atherogenenic
cell proliferation; elevated levels of fibrinogen are associated with coronary disease
and stroke [41,42].

Methods

Design/participants

The English Longitudinal Study of Ageing (ELSA) is an ongoing panel study of a nationally
representative sample of the English population living in households. The original
ELSA cohort consists of men and women born on or before 29 February 1952. The sample
was drawn from households that had participated in the Health Survey for England (HSE)
in 1998, 1999, and 2001. For the present analyses, data from the first wave (baseline,
2002-2003) and second wave (2004-2005) were used. The first and second wave involved
a face-to-face interview. The second wave also included a clinical assessment by a
nurse. This is the only wave containing the objective health assessment and blood
analysis data that is currently available for public use. Overall, 10,770 participated
in wave 1 (response rate 65.7%). Of these, 8,688 people participated in wave 2 (82%)
and 7,433 participants were willing to have a nurse visit. Of these, 6,649 people
consented to a blood sample.

Valid blood samples are available for 5,884 people of which 4,432 (75%) were fasting.
Fasting blood samples were taken for most respondents under the age of 80 except people
who had known diabetes and were on treatment, or whose heath the nurse was concerned
about. Subjects were considered to have fasted if they had not had food or drink for
a minimum of 5 hours prior to the blood test. However, there was no considerable differences
in the mean (Chi square test) for those who had fasted (fibrinogen mean = 3.27 and
SD = 0.0147; hsCRP mean = 2.52 and SD = 0.045) and for those who had not fasted (fibrinogen
mean = 3.33 and SD = 0.019; hsCRP mean = 2.703 and SD = 0.058). Because this is a
prospective population study (n = 8,688), due to the length of fieldwork (July 2004-
July 2005) and the overall fieldwork capacity, it was not possible to allow for circadian
effects by restricting nurses to, for example, morning-only appointments. While hsCRP
has no circadian or seasonal variation [43,44], the literature shows that for fibrinogen the proportion of variation attributed
to the diurnal, seasonal, and processing effects was only 2% [45].

Biological data were missing for participants who did not consent to give blood (participants
recently had a blood test, disliked needles or had previous difficulty with venipuncture,
n = 993), were ineligible (participants with clotting and bleeding disorders, or taking
anti-coagulant medication, n = 351) or for whom attempts to obtain a blood sample
were unsuccessful (incomplete/partial sample taken, insufficient blood for test or
no suitable/palpable vein/collapsed vein, n = 360). The analysis of the blood data
was carried out in the Royal Victoria Infirmary (Newcastle-upon-Tyne, UK). Both the
HSE and ELSA employed the same laboratory and the same guidelines and protocols for
the blood analysis. Detailed information on the technicalities of the blood analysis,
the internal control, and the external quality assessment are available in the 2004
HSE technical report [46]. Blood samples were analyzed for hsCRP and fibrinogen. Analysis of hsCRP levels from
serum was performed using the N Latex high sensitivity CRP mono immunoassay on the
Behring Nephelometer II analyser. The limit of detection was 0.17 mg/l and the coefficient
of variation (CV) was less than 6% for this assay. Fibrinogen levels were determined
using the Organon Teknika MDA 180 analyser, using a modification of the Clauss thrombin
clotting method, with a CV of less than 10%. These are acceptable limits in a large
population based sample. Blood pressure was recorded as the average of three seated
blood pressure readings (Omron HEM-907 blood pressure monitor).

In comparison with the overall sample (Chi square tested), the sub-group of people
who donated blood were younger (mean age 66 years old vs. 69 years), had a lower prevalence
of morbidity (39.1 vs. 26.2%), better self-reported health (75.3% vs. 60.5%) and better
health behaviours including lower rates of smoking (18.9% vs. 16.9%) and were less
sedentary (reported no frequency of physical activity 6.5% vs. 15%). However, social
engagement variables were not different between respondents who agreed to blood donation
and those for whom blood was not available for analysis.

In order to account for non-response to blood sample, weights were used which aimed
at reducing any bias arising from differential non-response between completion of
the nurse visit and giving a blood sample [47]. Using these weights allows correction for non-response at interview, nurse visit,
and in providing a non-fasting blood sample.

The final weights used thus incorporate adjustment for four levels of attrition/non-response:
1) from initial sample (HSE) to wave 1; 2) from wave 1 to wave 2; 3) from interview
at wave 2 to the nurse visit; and 4) non-response to blood donation. These weights
attenuate the potential selection biases due to attrition at different stages and
should ensure that the weighted data will be representative of the English population
living in the community who are over 50 years-old [48]. Details on the calculations of weights are presented in the ELSA technical report
[48].

Measurements

Cardiovascular risk markers

Cardiovascular risk variables were dichotomized. Hypertension is defined as SBP and DBP ≥ 140/90 mmHg [49] or SBP ≥ 140 (isolated systolic hypertension) or using hypertensive medication. Obesity was measured by body mass index (BMI), which was dichotomized by means of a cut-off
point of ≥ 30 kg/m2. For both hsCRP and fibrinogen [50], clinical cut-off points were used; hsCRP >3.0 mg/l was interpreted as high risk as it corresponds approximately to the highest
tertile of hsCRP in the adult population [50]. Cases with hsCRP higher than 10 mg/L were excluded from the hsCRP analysis because
such levels reflect an acute infection or inflammation other than those due to cardiovascular
disease [51]. For fibrinogen, values >4.0 g/L are a valid clinical cut-off and correspond to the highest quartile
concentration in the adult population [52].

Social engagement

Three different dimensions of social engagement were examined. Social participation was measured as a count of seven activities in which the respondent reported current membership or participation in any of a list of groups and associations divided into:
(1) political, trade union or environmental group; (2) tenants' groups, residents'
groups or neighbourhood watch; (3) church or other religious organization; (4) charitable
associations; (5) an education, arts or music group or evening class; (6) social club
(e.g. Rotary Club, elderly lunch group, women's group); and (7) any other organisations,
clubs or societies. The social participation raw score therefore ranges from 0 to
7. This was standardized as a Z-score. Scores range from -0.899 to 4.202 with weighted
mean of -0.087 (SD = 0.953). Higher scores indicate greater social participation.
Social ties were measured by a count of the number of children, relatives and friends the participant
felt close to ("How many of your children/relatives/friends would you say you have
a close relationship with?"). The final score was standardized and its value was averaged
across the ties that were relevant for a given respondent. Scores range from -1.256
to 1.533 with weighted mean of -0.090 (SD = 0.301). Emotional support from spouse, children, relatives and friends was measured by the following three questions:
a) How much respondents feel their spouse/partner (children/relatives/friends) understand(s)
their feelings; b) How much respondents can rely on their spouse/partner (children/relatives/friends)
if they have a serious problem; and c) How much respondents can open up to their spouse/partner
(children/relatives/friends) if they need to talk. The responses for each item range
from 0 (not at all) to 3 (a lot). Responses to all twelve questions were added up
to a summary score (Cronbach's alpha was 0.88). The emotional support scale was constructed
by standardizing and then averaging across the relevant item scores. Standardized
scores range from -2.409 to 0.1838 with weighted mean of -0.174 (SD = 0.554). Marital status was dichotomized as married (or cohabiting) and not married (never married, separated
or divorced, and widowed).

Demographic and socio-economic variables included age (in years), age squared, sex
(male as reference category), and education measured as the highest qualification
participants obtained, and categorized into four groups (no education, primary, secondary
and tertiary level).

Health behaviours

Smoking was coded as never smoked and ever smoked (ex-smoker or current smoker). Self-reported
physical exercise was classified as none, light, moderate and vigorous activity at
least once a week.

Co-morbidity

Physical function was assessed by dichotomizing the Activities of Daily Living into
"0 ADL", reporting no ADL difficulties and ""≥ 1 ADL", reporting one or more ADL difficulties.
Known cardiovascular disease was assessed by self-reported angina, myocardial infarction,
diabetes, stroke, heart failure, heart murmur, abnormal heart rhythm, and ischaemic
heart disease. Other major chronic diseases include self-reported chronic lung disease,
asthma, arthritis, osteoporosis, cancer, and Parkinson's disease. These variables
are dichotomized into "0 conditions" and "≥1 conditions". Depression was measured
by the 8-item Center for Epidemiologic Studies Depression Scale (CES-D) with a cut-off
point of 3 or more depressive symptoms [53] (<3 = non depressive, ≥3 = depressive).

Statistical Analysis

We used Spearman's rho to test for independence among social engagement variables.
The correlations between social participation and social ties (r = 0.15, p < 0.001),
and social participation and emotional support (r = 0.19, p < 0.001) were weak in
strength. Correlation between social ties and emotional support was moderate in strength
(r = 0.32, p < 0.001). Correlations between marital status and emotional support was
moderate in strength (r = 0.29, p < 0.001), while correlation between marital status
and social participation (r = 0.04, p < 0.001), and marital status and social ties
were weak in strength (r = 0.05, p < 0.001). Therefore, objective and subjective measurements
were not strongly correlated and, since they are conceptually distinct, we expect
that these four dimensions would have independent associations with cardiovascular
risk markers.

Using logistic regression, each cardiovascular risk factor (hypertension, BMI, fibrinogen,
and hsCRP) at wave 2 was regressed on the complete set of social engagement variables
at baseline (social participation, social ties, marital status and emotional support).
The independent effect of each of the social engagement variables was examined by
putting all the social engagement variables and confounding factors (age, gender,
education, co-morbidity and behavioral risk factors) into a single model. Seasonality
was adjusted for fibrinogen. Age squared was used to test for the non-linear relationship
between age and the outcome variables, and an interaction term between sex and age
was also included. The result of Goodness-of-fit tests (such as Akaike Information
Criterion- AIC and Bayesian Information Criterion-BIC) supported the model with interaction
and quadratic term over the nested model (with no interaction and quadratic term).
Data were weighted for panel attrition.

Results

Table 1 presents characteristics of the sample at baseline. The sample was composed of 53.4%
women and 46.6% men. The median age was 65.4 years (66.3 and 64.3 years for women
and men respectively). Sixty seven percent were married, and 40.5% had a primary education.
Thirty-seven percent reported no social participation, and 15.1% of the respondents
reported that they did not have children, relatives or friends that they felt close
to. Nighteen percent reported having cardiovascular morbidity, 39.7% reported having
non-cardiovascular chronic conditions, 29.9% reported difficulties with at least one
ADL, and 22.9% had depressive symptoms. Approximately 8% were relatively sedentary,
reporting no physical activity and 17.5% were smokers.

Table 1. Descriptive characteristics of the sample at baseline and CV risk factors at wave
2

Tables 2 and 3 shows the odds ratios (OR) and 95% confidence intervals (CIs) from logistic regression.
The results of these tables show whether baseline social engagement predicted the
cardiovascular risk factors at follow-up. First, we fitted a model controlling for
age, gender, education and co-morbidity (physical function, depression, cardiovascular
and chronic disease). In addition, behavioral risk factors (smoking, and physical
activity) known as confounders or mediators were adjusted in model 2.

In model 1, social participation was inversely associated with all four of the CV
risk markers (p < 0.05). For example, an increase of one standard deviation in social
participation was associated with about 7% lower odds of having hypertension, 11%
lower odds of being obese, and 10% and 12% lower odds of having higher levels of hsCRP
and fibrinogen, respectively. Being married was inversely associated with hypertension
and fibrinogen; being married would reduce the odds of having hypertension by 15%,
and the odds of elevated levels of fibrinogen by 16%.

Model 2 assesses the roles of behavioral factors as potential mediators or confounders
of the relationship between social engagement and CV risk factors. When behavioural
factors are controlled for, the associations between social participation and hypertension
and BMI remained unchanged. However, behavioral factors attenuated the results for
hsCRP (from 10% to 7%), and for fibrinogen (from 12% to 8%).

We also performed analysis without adjusting for the weights (results upon the request).
The results were similar and remained significant for those variables discussed in
the main text. In addition, to examine whether social engagement protects against
CV risk factors for those with pre-existing CVD, we constructed a version of model
2 with interaction terms. In those who had a pre-existing CVD, social ties had a protective
effect by lowering the hsCRP level (OR = 0.84, 95% CI: 0.716-0.995) and emotional
support increased the odds of being obese (OR = 1.58; 95% CI: 0.998-2.50). The other
dimensions of social engagement such as marital status and social participation were
not significant.

Discussion and Conclusions

Previous studies [5,19,54,55] examining objective aspects of social engagement (i.e. social participation and social
ties) found no consistent association between inflammatory markers (hsCRP and fibrinogen)
for older and younger women and younger men. The authors recommended that subjective
aspects of social engagement (such as emotional support) should be addressed in further
studies in order to provide insight into the role of inflammatory markers as biological
mediators between social engagement and cardiovascular disease. In addition, the way
that the social engagement variable was constructed in the previous studies made it
difficult to identify which particular aspects of people's social relationships are
associated with cardiovascular disease. This paper addressed this issue by incorporating
both objective and subjective measurements. Furthermore, this paper explored how social
engagement may protect against cardiovascular disease by examining its association
with cardiovascular risk factors.

Results indicate that within the objective measures, behavioral factors may mediate
the relationship between social participation and inflammatory markers i.e., the risks
of having higher concentrations of inflammatory markers may operate partially through
health behaviours. Conversely, for BMI and hypertension, social participation seems
to operate distinctly from behavioral factors and is an independent predictor of CV
risk markers.

Marriage is associated with hypertension and it is not mediated by behavioral factors.
Contrary to what has been suggested in the literature, social ties and emotional support
were not significant for CV risk factors [19]. We also tested whether emotional support mediates the relationship between social
ties and CV risk factors, but could not find strong evidence of such mediation. Additional
analysis was performed (not shown) to include measures of loneliness (only available
at wave 2). However, controlling for depression (CES-D minus the loneliness item),
the effect of loneliness was not significant.

Successive meta-analysis and prospective studies show evidence that depression is
associated with an increased risk of all-cause and cardiovascular death and that this
risk is particularly marked in depressive participants with co-morbid CHD [56-59]. However, the association between inflammatory markers and depression have been unclear
[60]. In this study, only fibrinogen was modestly associated with depression but not hsCRP.
Other studies, such as the Longitudinal Aging Study Amsterdam found similar results,
with no association between CRP and depression [61]. Therefore, the mechanisms linking depression to inflammatory markers are still poorly
understood. Meta-analysis in the future would help to clarify these contradictory
findings. Some limitations of how depressive symptoms were measured in ELSA need to
be also considered. The reduced 8 items of CES-D scale assesses depressive symptoms
rather than clinical depression. CES-D is therefore not a diagnostic test of depression
but poor scores are indicative of possible depression.

A recent study on social participation [62] did not find any consistent association with CV risk factors. However, the study
compared the mean scores of the CV risk markers by social participation adjusted only
for age and social class. Our study adjusted for various indicators of comorbidity
and behavioral factors to reduce the likelihood that the observed relationship between
social engagement and CV risk factors was a spurious one.

The findings suggest that participation in social, civic or political activities may
have an important effect on lowering CV risk factors. Previous research has found
that social participation has an impact on physical and mental health [63-65], survival at older ages [66], and is inversely associated with plasma fibrinogen [67,68]. Participation in political, social or civic activities provides social contacts
and gives rise to meaningful social roles which in turn provide a sense of value,
belonging and attachment in the community [28]. Social participation may give meaning and purpose to life through the fulfillment
of various social roles [69], thus lowering the levels of psychological distress [66]. Social participation may facilitate access to health information and services, and
provide access to resources such as information, transportation, and emotional support
[21]. It may even exert social control by encouraging health promoting behaviors such
as exercise, diet or discouraging health damaging behaviors such as smoking, excessive
eating, alcohol consumption and drug abuse [70].

The results also show that marriage was associated with hypertension. The protective
relationship between marriage and morbidity/mortality from cardiovascular disease
has been established in many studies [71]. Marriage may reduce stress and stress related illness [22], by attenuating the effects of stress on cardiovascular hyper-reactivity and on exaggerated
sympathetic nervous system activity [71].

This study has both strengths and limitations. Strengths include a large representative
sample of the non-institutionalized older population from which the findings can be
generalized, the use of four separate indicators of social engagement, and the careful
direct measurement of a range of relevant and previously validated cardiovascular
risk factors. The limitations are firstly that causality cannot be inferred from cross-sectional
data analysis (necessitated by the fact that availability of health measurement and
blood data is currently limited to a single wave of the study). Secondly, despite
the fact that we controlled for physical activities and that social participation
was not correlated with physical activities, one could argue that social participation
is actually measuring physical activities in ways not otherwise controlled for. We
tested whether some of the social participation items such as participation in tenants'
groups or neighbourhood watch might incorporate some amount of physical activity.
A correlation test was carried out on the relationship between physical activities
and each type of social participation, but only the item referring to "attending education,
arts or music groups or evening class" was weakly correlated (r = 0.127, p < 0.001).
The other activities were not correlated. In addition, in model 2 presented in the
paper, social engagement and physical activity were entered simultaneously and both
variables were significant. This result adds to our confidence that these variables
are independent predictors of CV risk factors and the effect of social participation
is not due to the impact of physical activity. Third, although we adjusted for an
extensive range of health factors, one could argue that social participation is actually
measuring health status in ways not otherwise controlled for. Future analyses of forthcoming
panel data will allow us to explore this and draw stronger causal inferences from
further waves.

This article has explored the relationships between different aspects of social engagement
and cardiovascular risk factors. Examination of different dimensions of social engagement
suggests that we can identify more precise biological pathways through which social
engagement influences cardiovascular disease. The analysis advanced here, it is hoped,
will be of relevance to scholars working at the intersection of the social and biomedical
sciences, who are seeking to understand the complex interactions between social engagement
and CVD.

Competing interests

The authors declare that they have no competing interests.

Authors' contributions

YK performed the statistical analysis, interpreted the results and drafted the manuscript.
BJW and VT participated in interpretation of the results and drafting the manuscript.
RK was responsible for the study interpretation and manuscript write-up. All authors
read and approved the final manuscript.

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